Ostadalova I, Ostadal B, Kolár F, Parratt J R, Wilson S
Institute of Physiology, Academy of Sciences of the Czech Republic, Prague, Czech Republic.
J Mol Cell Cardiol. 1998 Apr;30(4):857-65. doi: 10.1006/jmcc.1998.0653.
Although there is much information on ischaemic preconditioning in the adult myocardium, this phenomenon has not yet been investigated in neonatal hearts. To examine the early development of cardiac tolerance to ischaemia and the possible protective effects of preconditioning, rat hearts isolated on days 1, 4 and 7 of postnatal life were perfused (Langendorff) with Krebs-Henseleit solution at constant pressure, temperature (37 degrees C) and rate (200 beats/min). Developed force (DF) of contraction was measured by an isometric force transducer, and analysed using an on-line computer. Hearts were exposed to 40 or 60 min of global ischaemia followed by 30 min of reperfusion. Preconditioning was induced by three 3-min periods of global ischaemia, each separated by 5-min periods of reperfusion. Developmental changes in expression of protein kinase C (PKC) isoforms, and their activation following preconditioning, were estimated using Western blot analysis. Recovery of contractile function during reperfusion decreased from day 1 (48 +/- 2%) to day 4 (42 +/- 1%) and day 7 (33 +/- 2%). Preconditioning failed to improve ischaemic tolerance on day 1 (46 +/- 2%) and on day 4 (43 +/- 3%), but pronounced effect was observed on day 7 (40 +/- 2%). Prolonging the period of sustained ischaemia from 40 to 60 min on day 1 did not lead to a better recovery of contractile function in preconditioned hearts. PKC isoforms alpha, delta, epsilon and zeta were expressed in the ventricular myocardium during the first week of life, but there was no evidence of translocation following preconditioning on day 7. It may be assumed that the decreasing tolerance of the heart to ischaemia during early postnatal life is counteracted by the development of an endogenous protection.
尽管关于成年心肌缺血预处理的信息很多,但这一现象尚未在新生心脏中进行研究。为了研究心脏对缺血耐受性的早期发育以及预处理可能的保护作用,对出生后第1、4和7天分离的大鼠心脏进行Langendorff灌注,采用Krebs-Henseleit溶液,保持压力、温度(37℃)和速率(200次/分钟)恒定。通过等长力传感器测量收缩期的发展力(DF),并使用在线计算机进行分析。心脏先经历40或60分钟的全心缺血,然后再灌注30分钟。预处理通过三个3分钟的全心缺血期诱导,每个缺血期之间间隔5分钟的再灌注。使用蛋白质印迹分析评估蛋白激酶C(PKC)亚型表达的发育变化及其在预处理后的激活情况。再灌注期间收缩功能的恢复从出生后第1天(48±2%)下降到第4天(42±1%)和第7天(33±2%)。预处理在出生后第1天(46±2%)和第4天(43±3%)未能改善缺血耐受性,但在第7天观察到明显效果(40±2%)。在出生后第1天,将持续缺血时间从40分钟延长至60分钟,预处理心脏的收缩功能并未得到更好的恢复。PKC亚型α、δ、ε和ζ在出生后第一周的心室心肌中表达,但在第7天预处理后没有易位的证据。可以推测,出生后早期心脏对缺血耐受性的降低被内源性保护机制的发展所抵消。
